Sng (soreness) is the unpleasant feeling caused by muscle acidosis. Although traditionally classified as pain, recent studies show that Sng is mediated by acid-sensing ion channel 3 (ASIC3) on proprioceptors instead of nociceptors. In this study, we compare neuropathways of the trigeminal sensory system in the Sng and inflammatory pain model. Consistent with previous studies, we observed ASIC3-dependent chronic behavioral hypersensitivity upon repeated acidic saline injection into the masseter muscle. Nevertheless, the behavioral hypersensitivity induced by mustard oil is ASIC3-independent. By comparing the c-Fos activation of secondary sensory neuron activation 7 days after the secondary injection between sng and pain models, neurons in the principal trigeminal nucleus (Pr5), spinal trigeminal nucleus caudalis (Sp5C), and spinal trigeminal nucleus oralis (Sp5O) were activated by acid injection through ASIC3, while only those in the Sp5C were activated by mustard oil. Finally, Cre-dependent Adeno-Associated Virus (AAV) with different fluorescent proteins was injected into Pr5 and Sp5C of the TRAP2 mice, in order to label the active neurons 7 days after repeated acidic saline intramuscular injection. Pr5 projects to the ventral posteromedial nucleus (VPM) which is different from Sp5C projection in the thalamus. Since the Pr5 and SP5C contain the secondary sensory neurons of proprioception and nociception respectively, our results demonstrate that Sng and inflammatory pain display very different neurocircuits in the trigeminal system.